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西班牙1a型丙型肝炎病毒患者中与elbasvir相关的NS5A耐药相关替代突变的流行情况。

Prevalence of relevant NS5A resistance-associated substitutions to elbasvir in genotype 1a hepatitis C virus patients in Spain.

作者信息

Palladino Claudia, Esteban-Cartelle Beatriz, Mate-Cano Irene, Sánchez-Carrillo Marta, Resino Salvador, Briz Verónica

机构信息

Instituto de Investigación del Medicamento (iMed.ULisboa), Facultad de Farmacia, Universidad de Lisboa, Lisboa, Portugal.

Unidad de Infección Viral e Inmunidad, Laboratorio de Referencia e Investigación de Hepatitis Virales, Centro Nacional de Microbiología, Instituto de Salud Carlos III, Majadahonda, Madrid, España.

出版信息

Enferm Infecc Microbiol Clin (Engl Ed). 2018 May;36(5):262-267. doi: 10.1016/j.eimc.2017.03.008. Epub 2017 May 15.

Abstract

Resistance-associated substitutions (RASs) to the new HCV NS5A inhibitor elbasvir may limit its efficacy and lead to virological failure in HCV-GT1a-infected patients. There are no data outside clinical trials evaluating their prevalence and impact in grazoprevir/elbasvir in GT1a-infected patients in Spain. A multicentre cross-sectional study of 632 initial patients was conducted. In 13 of these patients, the sample could not be amplified or a consensus sequence by Sanger sequencing could not be performed. Ultimately, 617 HCV-G1a-infected individuals treated at 84 Spanish hospitals from the 17 autonomous communities plus the 2 autonomous cities of Spain were analysed. HCV population sequencing was used to identify RAS to elbasvir and the mutational pattern and drug sensitivity were confirmed by geno2pheno[HCV]. Viruses bearing RASs to elbasvir were present in 6.2% of HCV-G1a infected patients. The most common RASs were the Y93C/H/N and Q30E/H/R (2.4% and 2.3%, respectively). Only 3.4% of the identified RASs to elbasvir conferred reduced susceptibility to elbasvir by geno2pheno[HCV], which exclusively identified the positions Q30H/R (n=7) and Y93C/H/N (n=8) as single mutations and Q30H+Y93H (n=4) and Q30R+Y93H (n=2) as double mutations as the major RASs to elbasvir. A lower prevalence of RASs to elbasvir was observed in our HCV-G1a Spanish cohort than reported previously in clinical trials evaluating patients from the USA. This information may be essential to guide the implementation of grazoprevir/elbasvir in Spain and to manage G1a-infected patients.

摘要

对新型丙型肝炎病毒(HCV)NS5A抑制剂艾尔巴韦的耐药相关替代(RASs)可能会限制其疗效,并导致HCV - GT1a感染患者出现病毒学失败。在西班牙,除了评估GT1a感染患者中艾尔巴韦的耐药率及其对glecaprevir/艾尔巴韦疗效影响的临床试验数据外,尚无其他相关数据。我们开展了一项针对632例初治患者的多中心横断面研究。其中13例患者的样本无法扩增,或无法通过桑格测序获得一致序列。最终,我们分析了来自西班牙17个自治区加2个自治市的84家医院收治的617例HCV - G1a感染个体。采用HCV群体测序来鉴定对艾尔巴韦的RASs,并通过geno2pheno[HCV]确认突变模式和药物敏感性。6.2%的HCV - G1a感染患者存在对艾尔巴韦的RASs。最常见的RASs是Y93C/H/N和Q30E/H/R(分别为2.4%和2.3%)。通过geno2pheno[HCV]鉴定,仅3.4%的已鉴定对艾尔巴韦的RASs使病毒对艾尔巴韦的敏感性降低,其仅将Q30H/R(n = 7)和Y93C/H/N(n = 8)位点的单突变以及Q30H + Y93H(n = 4)和Q30R + Y93H(n = 2)位点的双突变确定为对艾尔巴韦的主要RASs。在我们的西班牙HCV - G1a队列中,观察到的对艾尔巴韦的RASs发生率低于之前评估美国患者的临床试验报告。这些信息对于指导西班牙glecaprevir/艾尔巴韦的应用以及管理G1a感染患者可能至关重要。

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